解析 p62/Sqstm1 在自噬体选择性降解途径中对 Nrf2 激活的作用。

Dissection of the role of p62/Sqstm1 in activation of Nrf2 during xenophagy.

机构信息

Protein Metabolism Project, Tokyo Metropolitan Institute of Medical Science, Tokyo 156-8506, Japan.

Laboratory of Protein Metabolism, Tokyo Metropolitan Institute of Medical Science, Tokyo 156-8506, Japan.

出版信息

FEBS Lett. 2014 Mar 3;588(5):822-8. doi: 10.1016/j.febslet.2014.01.045. Epub 2014 Feb 1.

DOI:10.1016/j.febslet.2014.01.045

PMID:24492006

Abstract

Upon infection of a cell by Salmonella, p62/Sqstm1 assembles on the microbes; simultaneously, p62/Sqstm1 is phosphorylated at Ser351, leading to inactivation of Keap1, which is responsible for degrading Nrf2. Thus, cytoprotective Nrf2 targets are induced at the same time that autophagosomes entrap the microbes (xenophagy). However, the detailed role of p62/Sqstm1 during xenophagy has remained unclear. Here we show that translocation of p62/Sqstm1 to invasive Salmonella precedes Ser351 phosphorylation. Furthermore, in addition to Ser351 phosphorylation, oligomerization of p62/Sqstm1 is also required for localization of Keap1 onto microbes, which is followed by Nrf2 activation. Our data reveal the sequential dynamics of p62/Sqstm1 in response to bacterial infection.

摘要

当细胞被沙门氏菌感染时，p62/Sqstm1 聚集在微生物上；同时，p62/Sqstm1 在丝氨酸 351 处被磷酸化，导致负责降解 Nrf2 的 Keap1 失活。因此，同时诱导具有细胞保护作用的 Nrf2 靶标，同时自噬体捕获微生物（异噬作用）。然而，p62/Sqstm1 在异噬作用中的详细作用仍然不清楚。在这里，我们表明 p62/Sqstm1 向侵袭性沙门氏菌的易位先于丝氨酸 351 磷酸化。此外，除了丝氨酸 351 磷酸化之外，p62/Sqstm1 的寡聚化对于 Keap1 定位到微生物上也是必需的，随后 Nrf2 被激活。我们的数据揭示了 p62/Sqstm1 对细菌感染的反应的顺序动力学。

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解析 p62/Sqstm1 在自噬体选择性降解途径中对 Nrf2 激活的作用。

Dissection of the role of p62/Sqstm1 in activation of Nrf2 during xenophagy.

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